Lipids reverse supramolecular chirality and reduce toxicity of amyloid fibrils. Academic Article

abstract

• Abrupt aggregation of misfolded proteins is a hallmark of many medical pathologies including diabetes type 2, Alzheimer and Parkinson diseases. This results in the formation of amyloid fibrils, protein aggregates with distinct supramolecular chirality. A growing body of evidence suggests that lipids can alter rates of protein aggregation. In this study, we investigated whether lipids could alter the supramolecular chirality of amyloid fibrils. We found that if present at the stage of protein aggregation, phospho- and sphingolipids uniquely reversed supramolecular chirality of insulin and lysozyme fibrils. Furthermore, amyloid fibrils with opposite supramolecular chirality exerted distinctly different cell toxicity. Specifically, insulin and lysozyme fibrils with reversed supramolecular chirality were less toxic to cells than the aggregates with normal supramolecular chirality. These findings point on the important role of lipids and supramolecular chirality of amyloid fibrils in the onset and progression of amyloid diseases.

authors

• Kurouski, Dzmitry

published proceedings

• FEBS J

altmetric score

• 3.1

author list (cited authors)

• Rizevsky, S., Zhaliazka, K., Matveyenka, M., Quinn, K., & Kurouski, D.

citation count

• 3

publication date

• December 2022

publisher

• Wiley  Publisher

keywords

• Amyloid
• Amyloid Fibrils
• Insulin
• Lysozyme
• Protein Aggregates
• Supramolecular Chirality
• Toxicity
• Vcd

Digital Object Identifier (DOI)

• 10.1111/febs.16564

start page

• 7537

end page

• 7544

volume

• 289

issue

• 23

URL

• http://dx.doi.org/10.1111/febs.16564